Temporal Signal Pattern Recognition in Mass Spectrometry: A Method for Rapid Identification and Accurate Quantification of Biomarkers for Inborn Errors of Metabolism with Quality Assurance.
Alicia DiBattistaNathan McIntoshMonica LamoureuxOsama Y Al-DirbashiPranesh ChakrabortyPhilip Britz-MckibbinPublished in: Analytical chemistry (2017)
Mass spectrometry (MS)-based metabolomic initiatives that use conventional separation techniques are limited by low sample throughput and complicated data processing that contribute to false discoveries. Herein, we introduce a new strategy for unambiguous identification and accurate quantification of biomarkers for inborn errors of metabolism (IEM) from dried blood spots (DBS) with quality assurance. A multiplexed separation platform based on multisegment injection-capillary electrophoresis-mass spectrometry (MSI-CE-MS) was developed to provide comparable sample throughput to flow injection analysis-tandem MS (FIA-MS/MS) but with greater selectivity as required for confirmatory testing and discovery-based metabolite profiling of volume-restricted biospecimens. Mass spectral information is encoded temporally within a separation by serial injection of three or more sample pairs, each having a unique dilution pattern, alongside a quality control (QC) that serves as a reference in every run to facilitate between-sample comparisons and/or batch correction due to system drift. Optimization of whole blood extraction conditions on DBS filter paper cut-outs was first achieved to maximize recovery of a wide range of polar metabolites from DBS extracts. An interlaboratory comparison study was also conducted using a proficiency test and retrospective neonatal DBS that demonstrated good agreement between MSI-CE-MS and validated FIA-MS/MS methods within an accredited facility. Our work demonstrated accurate identification of various IEM based on reliable measurement of a panel of primary or secondary biomarkers above an upper cutoff concentration limit for presumptive screen-positive cases without stable isotope-labeled reagents. Additionally, nontargeted metabolite profiling by MSI-CE-MS with temporal signal pattern recognition revealed new biomarkers for early detection of galactosemia, such as N-galactated amino acids, that are a novel class of pathognomonic marker due to galactose stress in affected neonates.
Keyphrases
- mass spectrometry
- liquid chromatography
- capillary electrophoresis
- ms ms
- high resolution mass spectrometry
- high resolution
- tandem mass spectrometry
- gas chromatography
- high performance liquid chromatography
- deep brain stimulation
- ultra high performance liquid chromatography
- single cell
- high throughput
- simultaneous determination
- quality control
- liquid chromatography tandem mass spectrometry
- solid phase extraction
- ultrasound guided
- multiple sclerosis
- bioinformatics analysis
- small molecule
- patient safety
- big data
- emergency department
- healthcare
- quality improvement
- magnetic resonance imaging
- cross sectional
- preterm infants
- amino acid
- social media
- deep learning
- ionic liquid
- artificial intelligence
- anaerobic digestion
- magnetic resonance
- sensitive detection
- heat stress